Friday, May 26, 2006

The Neurocritic has wondered why hippocampal neurogenesis has been touted as THE therapeutic sequela of antidepressant treatment ever since it was discovered as an interesting "side effect" of SSRI administration in rats. The hippocampus hasn't exactly been associated with mood regulation (the orbitofrontal cortex, sad cingulate, and amygdala, much more likely). Yes, it's thought that depressed people are more stressed, and stress is bad blah blah glucocorticoids blah blah hippocampus... other than that, is there any evidence that damaged hippocampi cause mood disorders? in focally-lesioned rodents? in amnesic humans? Could it be that hippocampal circuitry is more sensitive to a variety of insults (e.g., anoxic-ischemic events, excessive glucocorticoid levels, etc) and therefore, its integrity is a sensitive marker for some of the pathological cellular effects of stress-induced depression? Thus, fixing the ailing hippocampus itself may not be what causes remission of major depressive episodes.

And about that bureau genesis... what is that? A really brief bible placed by the Gideons in motel drawers? Oh, what? it's neurogenesis? . . . Never mind!

And about that neurogenesis. . . What do these new neurons do in adult humans? Are they fully functional?

Anyway, a new study touts neural progenitor cells as the key step for Prozac efficacy, as explained by this New Scientist article:

Prozac, one of the most common drug treatments for depression, acts by stimulating the growth of new neurons in the hippocampus. Grigori Enikolopov and his team from Cold Spring Harbor Laboratory in New York wanted to narrow down which steps in neurogenesis the drug was influencing. So they created mice with nuclei in their nerve cells that glow green during neurogenesis, making it easy to count and compare the number of developing neurons.

By tracking other factors associated with different stages of neurogenesis, Enikolopov's team found that only one step was actually influenced by Prozac: amplifying the neural progenitor cell, just downstream of the stem cell (see article in PNAS).

In the figure below, the blue arrow shows the step at which fluoxetine has its effect (Encinas et al., 2006).

...We have generated a reporter mouse line, which allows identification and classification of early neuronal progenitors. It also allows accurate quantitation of changes induced by neurogenic agents in these distinct subclasses of neuronal precursors. We use this line to demonstrate that the selective serotonin reuptake inhibitor antidepressant fluoxetine does not affect division of stem-like cells in the dentate gyrus but increases symmetric divisions of an early progenitor cell class. We further demonstrate that these cells are the sole class of neuronal progenitors targeted by fluoxetine in the adult brain and suggest that the fluoxetine-induced increase in new neurons arises as a result of the expansion of this cell class. This finding defines a cellular target for antidepressant drug therapies.

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About Me

Born in West Virginia in 1980, The Neurocritic embarked upon a roadtrip across America at the age of thirteen with his mother. She abandoned him when they reached San Francisco and The Neurocritic descended into a spiral of drug abuse and prostitution. At fifteen, The Neurocritic's psychiatrist encouraged him to start writing as a form of therapy.